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Fosfluconazole

Base Information
  • Chemical Name:Fosfluconazole
  • CAS No.:194798-83-9
  • Molecular Formula:C13H13F2N6O4P
  • Molecular Weight:386.255
  • Hs Code.:
  • UNII:3JIJ299EWH
  • DSSTox Substance ID:DTXSID3048601
  • Nikkaji Number:J1.645.469I
  • Wikipedia:Fosfluconazole
  • Wikidata:Q1439361
  • NCI Thesaurus Code:C81503
  • ChEMBL ID:CHEMBL1908301
  • Mol file:194798-83-9.mol
Fosfluconazole

Synonyms:fosfluconazole

Suppliers and Price of Fosfluconazole
Supply Marketing:
Business phase:
The product has achieved commercial mass production*data from LookChem market partment
Manufacturers and distributors:
  • Manufacture/Brand
  • Chemicals and raw materials
  • Packaging
  • price
  • DC Chemicals
  • Fosfluconazole(INN) >98%
  • 250 mg
  • $ 900.00
  • Crysdot
  • Fosfluconazole 95+%
  • 25mg
  • $ 49.00
  • Crysdot
  • Fosfluconazole 95+%
  • 50mg
  • $ 88.00
  • Crysdot
  • Fosfluconazole 95+%
  • 100mg
  • $ 147.00
  • ChemScene
  • Fosfluconazole 98.08%
  • 25mg
  • $ 120.00
  • ChemScene
  • Fosfluconazole 98.08%
  • 10mg
  • $ 60.00
  • ChemScene
  • Fosfluconazole 98.08%
  • 100mg
  • $ 288.00
  • ChemScene
  • Fosfluconazole 98.08%
  • 50mg
  • $ 180.00
  • American Custom Chemicals Corporation
  • FOSFLUCONAZOLE 95.00%
  • 100MG
  • $ 2317.35
Total 52 raw suppliers
Chemical Property of Fosfluconazole
Chemical Property:
  • Appearance/Colour:White to off-white solid 
  • Vapor Pressure:1.18E-20mmHg at 25°C 
  • Melting Point:223-224° 
  • Refractive Index:1.683 
  • Boiling Point:701.5 °C at 760 mmHg 
  • PKA:1.44±0.10(Predicted) 
  • Flash Point:378.1 °C 
  • PSA:137.99000 
  • Density:1.7 g/cm3 
  • LogP:1.23970 
  • XLogP3:-0.6
  • Hydrogen Bond Donor Count:2
  • Hydrogen Bond Acceptor Count:10
  • Rotatable Bond Count:7
  • Exact Mass:386.07039624
  • Heavy Atom Count:26
  • Complexity:511
Purity/Quality:

99% *data from raw suppliers

Fosfluconazole(INN) >98% *data from reagent suppliers

Safty Information:
  • Pictogram(s):  
  • Hazard Codes: 
MSDS Files:

SDS file from LookChem

Useful:
  • Canonical SMILES:C1=CC(=C(C=C1F)F)C(CN2C=NC=N2)(CN3C=NC=N3)OP(=O)(O)O
  • Description Fosfluconazole is a phosphate prodrug of fluconazole, and it was launched in Japan as an intravenous injection for the treatment of candidiasis and cryptococcosis infections. Fluconazole, a triazole antifungal agent, is a selective inhibitor of fungal cytochrome P450 sterol C-14 alpha-demethylation, and it is widely used for the treatment of patients with serious systemic fungal infections. Fluconazole is marketed in both oral and intravenous formulations, the latter being a dilute (2 mg/ mL) infusion in saline due to the relatively poor water solubility of the drug. In patients needing high doses (>400 mg) of fluconazole, a drawback of the IV formulation is the requirement of a high-volume infusion, which is undesirable in critically ill patients in whom fluid overload must be avoided. Fosfluconazole is a prodrug with approximately 40-fold higher water solubility than fluconazole, thereby achieving a substantial reduction in infusion volume. It is prepared in three steps starting from fluconazole. In the first step, fluconazole is converted to its dibenzyl phosphite derivative by reaction with phosphorous trichloride and benzyl alcohol. Subsequent oxidation of the phosphite to the corresponding phosphate with hydrogen peroxide and cleavage of the benzyl protecting groups by hydrogenolysis affords fosfluconazole. In vitro, fosfluconazole is at least 25-fold less potent than fluconazole against single isolates of Candida species and Cryptococcus neoformans. In vivo, it is rapidly hydrolyzed to fluconazole by phosphatase enzymes and exhibits similar efficacy to fluconazole in experimental models of fungal disease. The hydrolysis potential of fosfluconazole was initially demonstrated in homogenates of kidney, lung and liver of rat, dog, and human. Subsequently, in clinical trials with healthy volunteers (n=24), fosfluconazole was shown to hydrolyze rapidly and almost completely to provide a 97% mean bioavailability of fluconazole. Less than 1% of the administered dose of fosfluconazole was excreted unchanged in the urine, with the majority (85.6%) of the dose eliminated as fluconazole. The terminal half-life was about 2.3 hours, and the volume of distribution was 0.2 L/kg. The time to reach steady state drug levels with 500 mg daily dose was about 10 days, which could be shortened to 3 days by administering loading doses of 1000 mgs on days 1 and 2 followed by 500 mg daily. Further studies showed that hepatic or renal impairment did not significantly alter the pharmacokinetic profile of fosfluconazole. In phase III studies in patients with deep-seated mycosis due to Candida or Cryptococcus (n=160), a 2-day loading dose regimen of fosfluconazole provided efficacy range of 73.8% (in Japanese patients) to 91.7% (patients of non-Japanese origin). The adverse events seen in these trials were similar to those previously known with fluconazole therapy and included rash (3.1%), abnormal liver function values (2.5%), asthma (1.9%), and lightheadedness (1.9%).
Technology Process of Fosfluconazole

There total 8 articles about Fosfluconazole which guide to synthetic route it. The literature collected by LookChem mainly comes from the sharing of users and the free literature resources found by Internet computing technology. We keep the original model of the professional version of literature to make it easier and faster for users to retrieve and use. At the same time, we analyze and calculate the most feasible synthesis route with the highest yield for your reference as below:

synthetic route:
Guidance literature:
With sulfuric acid; In water; at 5 ℃; for 1h;
Guidance literature:
With hydrogenchloride; In 1,4-dioxane; water; for 2h; Solvent; Reagent/catalyst; Reflux;
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